Cardiovascular and other medical implants fabricated from low-modulus Ti-Nb-Zr alloys to provide enhanced biocompatibility and hemocompatibility. The cardiovascular implants may be surface hardened by oxygen or nitrogen diffusion or by coating with a tightly adherent, hard, wear-resistant, hemocompatible ceramic coating. The cardiovascular implants include heart valves, total artificial heart implants, ventricular assist devices, vascular grafts, stents, electrical signal carrying devices such as pacemaker and neurological leads, defibrillator leads, and the like. It is contemplated that the Ti-Nb-Zr alloy can be substituted as a fabrication material for any cardiovascular implant that either comes into contact with blood thereby demanding high levels of hemocompatibility, or that is subject to microfretting, corrosion, or other wear and so that a low modulus metal with a corrosion-resistant, hardened surface would be desirable.

Patent
   5690670
Priority
Dec 21 1989
Filed
Jun 06 1995
Issued
Nov 25 1997
Expiry
Nov 25 2014
Assg.orig
Entity
Large
184
25
EXPIRED

REINSTATED
1. An expandable stent for supporting a blood, urinary, or gastrointestinal vessel from collapsing inward, the stent having enhanced hemocompatibility, comprising:
(a) a radially outwardlly expandable stent body for insertion in a tubular conduit of a living body, said stent body having outer surfaces and a longitudinal bore therethrough for receiving a means for expanding said stent body radially outwardly; and
(b) anchoring means on said outer surfaces for engaging said tubular conduit and anchoring said stent body in a radially outward expanded position thereby supporting said tubular conduit from collapsing inward;
the stent at least partially fabricated from a biocompatible and hemocompatible low elastic modulus metal alloy comprising:
(i) titanium; and
(ii) from about 10 wt. % to about 20 wt. % niobium or from about 35 wt. % to about 50 wt. % niobium;
wherein the alloy is free of toxic elements, except such amounts of said toxic elements as may occur as impurities in the alloy and as contaminants as a result of an alloying process.
11. An expandable stent for supporting a blood, urinary, or gastrointestinal vessel from collapsing inward, the stent having enhanced hemocompatibility, comprising:
(a) a radially outwardlly expandable stent body for insertion in a tubular conduit of a living body, said stent body having outer surfaces and a longitudinal bore therethrough for receiving a means for expanding said stent body radially outwardly; and
(b) anchoring means on said outer surfaces for engaging said tubular conduit and anchoring said stent body in a radially outward expanded position thereby supporting said tubular conduit from collapsing inward;
the stent at least partially fabricated from a biocompatible and hemocompatible low elastic modulus metal alloy comprising:
(i) titanium; and
(ii) niobium and tantalum, wherein the combined wt. % of niobium and tantalum is from about 10 wt. % to about 20 wt. % or from about 35 wt. % to about 50 wt. %;
wherein the alloy is free of toxic elements, except such amounts of said toxic elements as may occur as impurities in the alloy and as contaminants as a result of an alloying process.
2. The stent of claim 1, wherein said alloy further comprises an amount of zirconium sufficient to retard the transformation of beta.
3. The stent of claim 2, wherein the metal alloy comprises from about 0.5 to about 20 wt. % zirconium.
4. The stent of claim 2, further comprising a hardened outer surface layer on at least a portion of the stent, said layer formed on the stent by a process selected from the group consisting of oxygen diffusion hardening, nitrogen diffusion hardening, physical vapor deposition, and chemical vapor deposition.
5. The stent of claim 2, wherein the metal alloy comprises about 74 wt. % titanium, about 13 wt. % niobium, and about 13 wt. % zirconium.
6. The stent of claim 2, wherein the metal alloy comprises titanium, from about 10 to about 20 wt. % niobium, and up to about 20 wt. % zirconium.
7. The stent of claim 2, wherein the metal alloy comprises titanium, from about 35 to about 50 wt. % niobium, and up to about 20 wt. % zirconium.
8. The stent of claim 1, further comprising a hardened outer surface layer on at least a portion of the stent, said layer formed on the stent by a process selected from the group consisting of oxygen diffusion hardening, nitrogen diffusion hardening, physical vapor deposition, and chemical vapor deposition.
9. The stent of claim 1 or claim 2 or claim 8 or claim 4, wherein surfaces of the stent that come into contact with body tissue or fluid are at least partially coated with a composition selected from the group consisting of anticoagulants, antimicrobial agents, antibiotics, and medicaments.
10. The stent of claim 1 or claim 2 or claim 8 or claim 4, further comprising a lower friction wear-resistant outer surface layer on at least a portion of the stent, said lower friction wear-resistant outer surface layer produced by a process selected from the group consisting of boronation and silver doping.
12. The stent of claim 11, wherein said alloy further comprises an amount of zirconium sufficient to retard the transformation of beta.
13. The stent of claim 12, wherein the metal alloy comprises from about 0.5 to about 20 wt. % zirconium.
14. The stent of claim 12, further comprising a hardened outer surface layer on at least a portion of the stent, said layer formed on the stent by a process selected from the group consisting of oxygen diffusion hardening, nitrogen diffusion hardening, physical vapor deposition, and chemical vapor deposition.
15. The stent of claim 11, further comprising a hardened outer surface layer on at least a portion of the stent, said layer formed on the stent by a process selected from the group consisting of oxygen diffusion hardening, nitrogen diffusion hardening, physical vapor deposition, and chemical vapor deposition.
16. The stent of claim 11 or claim 12 or claim 15 or claim 14, wherein surfaces of the stent that come into contact with body tissue or fluid are at least partially coated with a composition selected from the group consisting of anticoagulants, antimicrobial agents, antibiotics, and medicaments.
17. The stent of claim 11 or claim 12 or claim 15 or claim 14, further comprising a lower friction wear-resistant outer surface layer on at least a portion of the stent, said lower friction wear-resistant outer surface layer produced by a process selected from the group consisting of boronation and silver doping.

This is a division of application Ser. No. 08/112,599 filed on Aug. 26, 1993, U.S. Pat. No. 5,477,864 which is a continuation-in-part of U.S. Ser. No. 08/036,414 filed on Mar. 24, 1993, U.S. Pat. No. 5,509,933 which is in turn a continuation-in-part of U.S. Ser. No. 07/986,280, filed on Dec. 7, 1992, abandoned, which is a continuation-in-part of Ser. No. 07/647,453, filed on Jan. 28, 1991, issued as U.S. Pat. No. 5,169,597, which is in turn a continuation of U.S. Ser. No. 07/454,181, filed on Dec. 21, 1989, abandoned.

1. Field of the Invention

This invention relates to a range of cardiovascular and other implants fabricated of metallic alloys of enhanced hemocompatibility that can optionally be surface hardened to provide resistance to wear, or cold-worked or cold-drawn to reduce elastic modulus, if necessary. More specifically, the invention is of synthetic heart valves, ventricular assist devices, total artificial hearts, stents, grafts, pacers, pacemaker leads and other electrical leads and sensors, defibrillators, guide wires and catheters, and percutaneous devices fabricated of Ti-Nb-Zr alloys.

2. Description of the Related Art

Cardiovascular implants have unique blood biocompatibility requirements to ensure that the device is not rejected (as in the case of natural tissue materials for heart valves and grafts for heart transplants) or that adverse thrombogenic (clotting) or hemodynamic (blood flow) responses are avoided.

Cardiovascular implants, such as heart valves, can be fabricated from natural tissue. These bioprostheses can be affected by gradual calcification leading to the eventual stiffening and tearing of the implant.

Non-bioprosthetic implants are fabricated from materials such as pyrolytic carbon-coated graphite, pyrolytic carbon-coated titanium, stainless steel, cobalt-chrome alloys, cobalt-nickel alloys, alumina coated with polypropylene and poly-4-fluoroethylene.

For synthetic mechanical cardiovascular devices, properties such as the surface finish, flow characteristics, surface structure, charge, wear, and mechanical integrity all play a role in the ultimate success of the device. For example, typical materials used for balls and discs for heart valves include nylon, silicone, hollow titanium, TEFLON™, polyacetal, graphite, and pyrolytic carbon. Artificial hearts and ventricular assist devices are fabricated from various combinations of stainless steel, cobalt alloy, titanium, Ti-6Al-4V alloy, carbon fiber reinforced composites, polyurethanes, BIOLON™ (DuPont), HEMOTHANE™ (Sarns/3M), DACRON™, polysulfone, and other thermoplastics. Pacers, defibrillators, leads, and other similar cardiovascular implants are made of Ni-Co-Cr alloy, Co-Cr-Mo alloy, titanium, and Ti-6Al-4V alloy, stainless steel, and various biocompatible polymers. Stents and vascular grafts are often made of DACRON™ stainless steel or other polymers. Catheters and guide wires are constructed from Co-Ni or stainless steel wire with surrounding polymer walls.

One of the most significant problems encountered in heart valves, artificial hearts, assist devices, pacers, leads, stents, and other cardiovascular implants is the formation of blood clots (thrombogenesis). Protein coatings are sometimes employed to reduce the risk of blood clot formation. Heparin is also used as an anti-thrombogenic coating.

It has been found that stagnant flow regions in the devices or non-optimal materials contribute to the formation of blood clots. These stagnant regions can be minimized by optimizing surface smoothness and minimizing abrupt changes in the size of the cross section through which the blood flows or minimizing other flow interference aspects. While materials selection for synthetic heart valves, and cardiovascular implants generally, is therefore dictated by a requirement for blood compatibility to avoid the formation of blood clots (thrombus), cardiovascular implants must also be designed to optimize blood flow and wear resistance.

Even beyond the limitations on materials imposed by the requirements of blood biocompatibility and limitations to designs imposed by the need to optimize blood flow, there is a need for durable designs since it is highly desirable to avoid the risk of a second surgical procedure to implant cardiovascular devices. Further, a catastrophic failure of an implanted device will almost certainly result in the death of the patient.

The most popular current heart valve designs include the St. Jude medical tilting disc double cusp (hi-leaf) valve. This valve includes a circular ring-like pyrolytic carbon valve housing or frame and a flow control element which includes pyrolytic carbon half-discs or leaves that pivot inside the housing to open and close the valve. The two leaves have a low profile and open to 85° from the horizontal axis.

Another popular heart valve is the Medtronic-Hall Valve wherein the flow control element is a single tilting disc made of carbon coated with pyrolytic carbon which pivots over a central strut inside a solid titanium ring-like housing. A third, less popular design, is the Omniscience valve which has a single pyrolytic disc as a flow control element inside a titanium housing. Finally, the Starr-Edwards ball and cage valves have a silastic ball riding inside a cobalt-chrome alloy cage. The cage is affixed to one side of a ring-like body for attachment to the heart tissue. More recent designs include trileaflet designs and concave bileaflet designs to improve blood flow.

From the point of view of durability, heart valves made of low-thrombogenic pyrolyte carbon could fail from disc or pivot joint wear or fracture related to uneven pyrolytic carbon coating, fracture of the ball cage, disc impingement, strut wear, disc wear, hinge failure, and weld failure. A more recent heart valve, the Baruah Bileaflet is similar to the St. Jude design but opens to 80° and is made of zirconium metal. The valve has worked well over its approximately two-year history with roughly 200 implants to date in India. This performance can be partly attributed to the lower elastic modulus of zirconium (about 90 GPa) and the resultant lower contact stress severity factor (Cc of about 0.28×10-7 m) when the disc contacts the frame. In contrast, pyrolytic constructions produce contact stress severity factors of about 0.54×10-7 m.

Although zirconium has worked well to date and can reduce contact stress severity, zirconium metal is relatively soft and sensitive to fretting wear. This is partly due to hard, loosely attached, naturally-present passive oxide surface films (several nanometers in thickness) which can initiate microabrasion and wear of the softer underlying metal. However, this naturally present zirconium oxide passive film is thrombogenically compatible with blood and the design is acceptable from a hemodynamic standpoint. Therefore, while the zirconium bileaflet valve appears to meet at least two of the major requirements for cardiac valve implants, namely blood compatibility and design for minimum stagnant flow regions, the use of soft zirconium metal leads to a relatively high rate of fretting wear and leads to the expectation that the valve may be less durable than one produced from materials less susceptible to fretting wear. Titanium and titanium alloys present a similar limitation, and Co-Cr-Mo, stainless steel, and Co-Ni alloys have much greater elastic modulus.

There exists a need for a metallic cardiac valve implant that is biocompatible, compatible with blood in that it does not induce blood clotting and does not form a calcified scale, that is designed to minimize stagnant flow areas where blood clotting can be initiated, that has a low elastic modulus for lower contact stress severity factors to ensure resistance to wear from impact, and that has a surface that is also resistant to microabrasion thereby enhancing durability.

Heart diseases, many of which cannot be cured by conventional surgery of drug therapy, continue to be a leading cause of death. For the seriously ill patient, heart replacement is often one of the few viable options available.

In 1988, the NHBLI began funding research and development for permanently implantable, electrically driven, total artificial hearts (TAHs). The pumping mechanism of the TAHs would be implanted into the chest cavity of the patient and the device would be powered by a battery pack and a small transformer, worn by the patient, which transmits energy to the heart with no physical connections through the skin. The NHBLI funded four separate groups: The Cleveland Clinic Foundation & Nimbus, Inc.; Pennsylvania State University & Sarns/3M; The Texas Heart Institute and Abiomed, Inc.; and the University of Utah. Consequently, four competing designs were developed.

The development of TAHs posed several issues. Firstly, it was necessary to duplicate the action of a human heart, ensure long-term reliability and biocompatibility, while producing a device that fits into the chest cavity in terms of both its total volume and the orientation of its connections to natural vessels in the body. Aside from the purely mechanical, wear, and power supply issues, it is also necessary that the design and materials prevent infection and thrombosis. Blood is a non-Newtonian fluid and its properties, such as viscosity, change with oxygen content, kidney function, and even the age of the patient. Further, plasma contains a suspension of fragile red blood cells which may be caught in artificial valves, or other mechanically stressful areas, thereby destroying these cells. It is therefore necessary to develop a TAH that does not stress blood components, and to fabricate the pump from materials that are not only biocompatible, but also "blood compatible" in the sense of minimizing damage to blood components and minimizing the formation of blood clots.

Many of the above comments also apply to ventricular assist devices (VADs), one of which is being developed by the Novacor Division of Baxter Health Care Corp. In the use of a VAD, the patient's heart remains in place while the VAD boosts the pumping pressure of the left ventricle of the heart. Consequently, the VAD is an assist device rather than a replacement. However, the VAD must be blood compatible for the same reasons as the total artificial heart.

There exists a need for a material that is lightweight, readily formable into complex shapes, biocompatible, and blood and tissue compatible with a hard surface that is resistant to abrasive wear, microfretting wear, and the corrosive effects of body fluids, for use in heart assist or replacement devices (including EMHs, VADs, and TAHs) to prolong the life of mechanical components while at the same time minimizing any deleterious effect on blood components.

The invention provides cardiovascular and other medical implants of a low modulus, biocompatible, hemocompatible, metallic alloy of titanium with niobium and optionally zirconium. The invention implants include heart valves, artificial hearts, ventricular assist devices, defibrillators, pacers, electrical leads, sensors, grafts, stents, and catheter devices. The invention also provides surface hardened versions of these devices produced by oxygen or nitrogen diffusion hardening to improve resistance to cavitation, microfretting wear, and impact-induced wear.

The inherently low modulus of Ti-Nb-Zr alloys, between about 6 to about 12 million psi depending on metallurgical treatment and composition, provide a more flexible and forgiving construct for cardiovascular applications while improving contact stress levels, valve closure, and the ability of leaves in certain valve designs to self-align with blood flow and reduce thrombodynamic effects.

The invention provides components for use in mechanical heart replacement or assist devices, such as external mechanical hearts (EMHs), total artificial hearts (TAHs), and ventricular assist devices (VADs), that are lightweight, while also being resistant to corrosive body fluids, mechanical wear, abrasive wear, and microfretting wear. Further, the components have much improved blood compatibility in the sense of reduced risk of thrombogenesis (blood clotting).

The preferred low modulus titanium alloys of the invention have the compositions: (i) titanium; about 10 wt. % to about 20 wt. % niobium; and optionally from about 0 wt. % to about 20 wt. % zirconium; and (ii) titanium; about 35 wt. % to about 50 wt. % niobium; and optionally from about 0 wt. % to about 20 wt. % zirconium. Tantalum can also be present as a substitute for Nb. These alloys are referred to herein as "Ti-Nb-Zr alloys," even though tantalum may also be present.

The exclusion of elements besides titanium, zirconium, and niobium, or tantalum results in an alloy which does not contain known toxins or carcinogens, or elements that are known or suspected of inducing diseases or adverse tissue response in the long term.

Without the presence of zirconium in the composition, the ability of the Ti-Nb-Zr alloy to surface harden during oxygen or nitrogen diffusion hardening treatments is more limited. Therefore, presence of zirconium is especially preferred when the alloy implant must be diffusion hardened. Other non-toxic filler materials such as tantalum, which stabilize the β-phase of titanium alloy, but do not affect the low modulus, i.e., maintain it at less than about 85 GPa, could also be added.

A porous coating, such as plasma-sprayed or sintered titanium or titanium alloy (including Ti-Nb-Zr alloy) beads or wire mesh may also be added to the implant's surfaces to improve tissue attachment, such as the formation of an endothelial cell layer, preferred in artificial heart, ventricular assist devices, grafts, and stent devices. Such coatings provide more favorable blood interaction and flow characteristics, and also tend to stabilize the implant with the body. Thus, such porous coatings may also be useful for connecting regions of these devices as well as for heart valves and grafts. Even though the application of such porous coatings usually requires sintering at relatively high temperatures, the properties of the Ti-Nb-Zr alloy that might affect its usefulness as an implant material are not adversely affected.

A better understanding of the present invention can be obtained when the following detailed description of the preferred embodiments is considered in conjunction with the following drawings, in which:

FIG. 1 shows a simplified representation of a ball valve, like the Starr-Edwards Valve.

FIG. 2 is a simplified representation of a disc valve.

FIG. 3 is a simplified representation of a tilting disc, single cusp valve like the Medtronic-Hall valve.

FIG. 4 is a simplified representation of a tilting disc, double cusp or bileaflet valve of the St. Jude or Baruah type.

FIG. 5 is a schematic diagram of the Penn State/Sarns/3M design total artificial heart.

FIG. 6 is a schematic diagram of the University of Utah total artificial heart.

FIG. 7 is a schematic diagram of the Cleveland Clinic/Nimbus, Inc. total artificial heart.

FIG. 8A is a schematic diagram, in cross section, of the Texas Heart Institute/Abiomed total artificial heart.

FIG. 8B is a side view, in cross section, of the Texas Heart Institute/Abiomed total artificial heart of FIG. 8A.

FIGS. 9A and B are schematic diagrams of end and front views, respectively, of a ventricular assist device.

FIG. 10 is a schematic diagram of a vascular graft of woven metallic wire composition.

FIG. 11A is a schematic diagram showing a balloon expandable stent positioned within a segment of a blood vessel to be propped open.

FIG. 11B is a schematic diagram showing a balloon expanding a stent into position within a blood vessel.

FIG. 11C is a schematic diagram of a stent expanded in a blood vessel.

FIG. 12A is a schematic diagram of the components of a defibrillator, showing power source, lead wire, and polymeric patch with coiled electrode.

FIG. 12B is a cross section of the lead wire of FIG. 12A.

FIG. 13A is a schematic diagram, in partial cross section, of the distal end of a guide wire.

FIG. 13B is a cross-section of the guide wire with coating thickness exaggerated.

FIG. 13C shows a catheter containing coiled wire and polymer wall.

FIGS. 14A-C are schematic diagrams of prior art pacemaker leads with polyurethane covering.

FIG. 14D is a schematic of an embodiment of the invention Ti-Nb-Zr pacemaker leads.

The implants of the invention are fabricated from an alloy containing titanium as a component. The preferred low modulus titanium alloys have the compositions: (i) titanium, about 10 wt. % to about 20 wt. % niobium, and optionally from about 0 wt. % to about 20 wt. % zirconium; and (ii) titanium, about 35 wt. % to about 50 wt. % niobium, and optionally from about 0 wt. % to about 20 wt. % zirconium.

In a preferred embodiment wherein the implants are surface hardened by oxygen or nitrogen diffusion, zirconium is beneficially present in amounts ranging from about 0.5 to about 20 wt. %.

Even though it is apparent that the titanium proportion of alloy used to make the invention implants could be less than 50 wt. %, nevertheless, for the purposes of this specification, it is referred to as a "Ti-Nb-Zr alloy" or a "titanium alloy." The alloy most preferably comprises about 74 wt. % titanium in combination with about 13 wt. % of zirconium and 13 wt. % of niobium. While tantalum may be substituted for niobium to stabilize β-phase titanium, niobium is the preferred component due to its effect of lowering the elastic modulus of the alloy when present in certain specific proportions. Other elements are not deliberately added to the alloy but may be present in such quantities that occur as impurities in the commercially pure titanium, zirconium, niobium, or tantalum used to prepare the alloy and such contaminants as may arise from the alloying process.

In the specification and claims, the term"high strength" refers to an alloy having a tensile strength above at least about 620 MPa.

The term "low modulus," as used in the specification and claims, refers to a Young's modulus below about 90 GPa.

Although the hot rolled, reheated, and quenched Ti-Nb-Zr alloy is a suitable implant material, its properties can be improved by forging or other metallurgical processes or an aging heat treatment or a combination of these. Aging treatment can increase the strength and hardness of the material, and reduce its elongation while maintaining a relatively low modulus of elasticity. The treatment can be varied to obtain the desired properties. U.S. Pat. No. 5,169,597 to Davidson, et al., hereby fully incorporated by reference, deals in more detail with the useful Ti-Nb-Zr alloys. Further, U.S. Ser. No. 08/036,414 U.S. Pat. No. 5,509,933, hereby fully incorporated by reference, teaches how to hot work Ti-Nb-Zr alloys to produce high strength, low modulus medical implants.

It may be desirable for other reasons, such as reducing microfretting wear between mating mechanical components, to surface harden the alloy implants using oxygen or nitrogen diffusion hardening methods, or coating with a hard wear resistant coating. In the latter event, the surface of the prosthesis may be coated with an amorphous diamond-like carbon coating or ceramic-like coating such as zirconium or titanium oxide, zirconium or titanium nitride, or zirconium or titanium carbide using chemical or plasma vapor deposition techniques to provide a hard, impervious, smooth surface coating. These coatings are especially useful if the prosthesis is subjected to conditions of wear, such as, for instance, in the case of mating parts in artificial hearts or ventricular assist devices, or as an electrically insulative coating on electrical leads (i.e., pacemaker, defibrillator, neurological, sensors) of Ti-Nb-Zr alloy.

Methods for providing hard, low-friction, impervious, biocompatible amorphous diamond-like carbon coatings are known in the art and are disclosed in, for example, EPO patent application 302 717 A1 to Ion Tech and Chemical Abstract 43655P, Vol. 101, describing Japan Kokai 59/851 to Sumitomo Electric, all of which are incorporated by reference herein as though full set forth.

A preferred process for oxygen diffusion hardening is described in U.S. Pat. No. 5,372,660, which is hereby fully incorporated by reference. Oxygen diffusion hardening according to this process requires the supply of oxygen, or an oxygen containing atmosphere, or compounds partially composed of oxygen, such as water (steam), carbon dioxide, nitrogen dioxide, sulfur dioxide, and the like. These substances are supplied to the implant to be hardened which is maintained at a temperature preferably between 200°C and 1200°C The amount of time required at a given temperature to effectively produce the surface and near-surface hardened implants is related exponentially, by an Arhennius-type relationship to the temperature. That is, shorter periods of time are required at higher temperatures for effective diffusion hardening. The resultant oxygen diffusion hardened implants are characterized in that the oxide film contains primarily a mixture of titanium and zirconium oxides in the implant surface. Niobium oxides may also be present. Immediately underlying this mixed-oxide film is sometimes a region of oxygen-rich metal alloy. Underlying the sometimes-obtained oxygen-rich alloy layer is the core Ti-Nb-Zr alloy. The interface between the sometimes-obtained oxygen-rich alloy layer and the oxide regions is typically zirconium-rich in comparison to the underlying Ti-Nb-Zr alloy. In a most preferred embodiment, the Tb-Ni-Zr alloy is subjected to temperature and an environment of argon gas that has been moisturized by bubbling through a water bath. The water vapor disassociates at the implant surface to produce oxygen which diffuses into the implant to produce the desired hardened surface.

Nitrogen diffusion processes can also be utilized in which nitrogen sources are provided instead of oxygen. These nitrogen diffusion surface hardening processes will tend to harden the metal alloy substrate in a similar manner to that of oxygen diffusion hardening or conventional oxygen hardening (which is also useful), and produce a yellow-orange insulative, wear-resistant surface nitride instead of the blue-black surface oxide which typically forms from the in situ oxygen diffusion hardening process.

Implants fabricated from the inventive alloy may be supplied with a porous bead or wire coating of titanium alloy of the same or different composition including pure titanium to allow endothelial cell attachment to blood-contacting flow surfaces or for stabilization of the implant in the body of the patient after implantation by tissue in growth into the porous structure. Such porous structures are normally attached to the implant surface by sintering or plasma spraying. Sintering involves heating the implant to above about 1250°C The mechanical properties of titanium alloys can change significantly due to substantial grain growth and other metallurgical factors arising from the sintering process. Thus, after sintering to attach the porous coating, it may be desirable in some instances to reheat the Ti-Nb-Zr implant, for example, to about 875°C (or above the β-transus) for 20-40 minutes then water quench before aging at about 500°C for about 6 hours to restore mechanical properties. If quenched adequately from the sintering temperature, it may be possible to go directly to the aging process. Art alternative method of attaching a porous coating is to simply plasma spray metal powder or micro-beads onto the implant's surface after appropriate mechanical and thermal treatments.

Further, the implants of the invention may optionally be surface coated with medicaments such as anti-inflammatory agents, anti-thrombus agents, antibiotics, proteins that reduce platelet adhesion, and the like to improve their acceptability in a living body.

In its simplest form, a synthetic cardiac valve includes a valve body for affixing the valve to the body tissue and through which blood flows, and a flow control element for allowing or blocking off blood flow. For instance, FIG. 4 shows a typical bileaflet valve having a valve body that includes a ring-like housing 400 with an inner ring 402 that has two flanges 404 each containing two slots for receiving hinges attached to leaflets. The flow control element of this valve comprises two leaflets 405, in the approximate shape of half discs, with hinge elements attached at diametrically opposite ends. These hinge elements fit within apertures or slots in the flanges 404 of the inner ring 402 and are able to rotate through less than 180°C in these apertures. Thus, in operation, the flow control elements are in the position shown in FIG. 4 with the valve open with blood flowing from top to bottom. When blood flow reverses and flows from bottom to top, the bileaflets 405 pivot about their hinges to close the apertures in the ring-like valve body. Consequently, there is a significant amount of movement about the hinge elements and slots where microfretting wear might be initiated. Furthermore, the bileaflet half disc flow control elements 405 may impinge upon the inner ring 402 of the valve body, thereby leading to cavitation or impact-induced wear.

The invention provides heart valves of various designs, exemplified in FIG. 1-4, each comprising parts subject to impact and wear that are fabricated from Ti-Nb-Zr alloy. More recent designs (not shown in the Figures) include concave bileaflet and trileaflet designs which are intended to improve blood flow. The heart valves are preferably subjected to a hardening process, such as oxygen or nitrogen diffusion hardening to produce a harder Ti-Nb-Zr surface that is resistant to microfretting wear at hinge points and impact wear at those locations where a flow control element impacts the valve body. Consequently, the invention valves have a longer cycle life than the currently used St. Jude, Omniscience, Starn-Edwards, Medtronic-Hall, or Baruah valves. Indeed, as mentioned before, the Baruah valve is currently fabricated of zirconium or zirconium alloys and would therefore be subject to relatively rapid wear because of the relative softness of zirconium and its alloys. The use of Ti-Nb-Zr alloy compositions also provides a low-thrombus, blood-compatible surface favorable in reducing the incidence of blood clots.

FIG. 5 is illustrative of the Penn State design which incorporates a stainless-steel roller screw 10 positioned between two flexible diaphragm blood pumps (right side pump 12 is shown, the other is within shell 8). A high speed, low torque brushless DC motor causes the roller screw 10 to turn thereby moving the roller screw shafts 16 linearly back and forth. To each end of the guide shaft 16 is attached a pusher plate 18. When the pusher plate 18 in the right side pump moves backward, blood is drawn into the pump space 14. At the same time, the pusher plate in the corresponding left side pump moves towards the left pushing blood out of its pump space. In this type of pump, the pusher plates 18 act against a flexible membrane 12, which is in contact with blood, and which can be inflated on the pump suction stroke and deflated on pump discharge stroke. The pusher plates are driven by the roller screw 10 and, thus, according to the invention, six revolutions of roller screw 10 are required for a full stroke with a motor speed of about 3,000 RPM. While planetary rollers are inserted between a roller screw nut and roller screw 10 to give rolling, not sliding contact and to spread mechanical load over many contact points, and while the entire roller screw system is hardened to minimize wear, the reliability of this system is improved by the use of the invention components. Thus, roller screw 10 and the roller-screw nut with which it is in rolling contact are both fabricated of Ti-Nb-Zr alloy and the surfaces are hardened or coated with a hard, tightly adherent coating. Further, the surfaces of the pump nozzles 2 shown as 4 and 6, connecting elements 20 and conduits 22, into and from which blood is continuously being pumped, is fabricated from Ti-Nb-Zr to reduce adverse reaction with blood tissue on those surfaces presented to blood components to minimize the potential for the formation of thrombus and blood clots.

FIG. 6 is a schematic cross-sectional diagram of the University of Utah electrohydraulic heart. This heart includes shells 50 and 52 with a pump motor 34 interposed between them. In this type of heart, a motor 20 is used to pressurize silicone oil in regions 22 and 24 on the undersides of flexible diagrams 26 and 28, respectively, to move blood in and out of the chambers 30 and 32 above the flexible diaphragms. For example, when motor 34 pressurizes silicone oil into chamber 22, then flexible diaphragm 26 expands upward and outwardly to push blood flow out of chamber 30 in direction 36. At the same time, silicon oil flows out of chamber 24 towards chamber 22 thereby allowing flexible diaphragm 28 to assume a natural position, shown in FIG. 2, and drawing blood into chamber 32 as shown from direction 38. Upon reversal of the direction of the bidirectional pump 34, the opposite effects are achieved.

Since the University of Utah pump is of a bidirectional design, and typically operates at speeds between 10,000-13,000 RPM in the high pressure direction and 5,000-8,000 RPM in the reverse, moving components of the pump are subject to microfretting and mechanical wear. Therefore, the invention components for the bidirectional axial flow pump 34 used in the University of Utah TAH design are fabricated from Ti-Nb-Zr alloy coated hardened or with a wear resistant, hard coating that is tightly adherent, to reduce wear of the high speed components. Further, surfaces 40, 41, 42 43, 44 and 45 are in direct contact with blood and are made of Ti-Nb-Zr alloy to improve blood compatibility and reduce the potential for thrombus and blood clotting. Thus, the shells of the heart 50 and 52 are also fabricated of Ti-Nb-Zr alloy to reduce thrombogenesis.

FIG. 7 is a schematic cross-sectional illustration of the Cleveland Clinic TAH which utilizes a motor to turn a gear pump 56 which provides hydraulic pressure at about 100 psi to cause reciprocal movement of actuators 58 which in turn drive pusher-plates 60 that act on flexible diaphragms 62 to pump the blood. The actuators 58 operate slidingly within guide sleeve 64 so that wear on contact surfaces between actuator and sleeve may be expected. Further, the TAH has a flow reversing valve 64 with machine elements, such as bearing surfaces, subject to wear when the TAH is in use. Thus, TAH elements that are subject to wear and that may be advantageously fabricated of Ti-Nb-Zr alloys that are then surface hardened and/or coated with a hard, wear resistant, tightly adherent coating, include the guide sleeve 64, the actuators 58, the pump's gear elements and shaft and the rotary valve 64. Moreover, to reduce the risk of erosion damage to the pump from cavitation, the pump housing 72 may likewise be fabricated of Ti-Nb-Zr alloys. Finally, internal surfaces 66, 68 of the heart housing 70 are in direct blood contact. Thus it is desirable to fabricate housing 70 from Ti-Nb-Zr to reduce the risk of thrombogenesis.

FIGS. 8A and B are schematic diagrams of the Texas Heart Institute/Abiomed TAH design which utilizes a d.c. motor to drive a miniature centrifugal pump 80 that rotates at about 6,000-8,000 RPM. This pump 80 pressurizes hydraulic fluid alternately into chambers 82 and 84 separated by septum 86 and enclosed by flexible diaphragms 88 and 90 respectively. As fluid is pumped into chamber 82, diaphragm 88 expands into heart space 92 forcing blood from this space. At the same time, fluid is pumped from chamber 84 causing diaphragm 90 to relax and expanding heart space 94, drawing blood into the TAH. The hydraulic flow is reversed by a two-position 4-way rotating valve 100 of radial configuration for compactness. Rotary valve 100 rotates within sleeves 102 and 104 at high speed so that contacting surfaces between the valve 100 and these sleeves are subject to wear. Further, rotary valve 100 rotates against seals 106 and wear may be expected at the contacting surfaces of the seals and the valve 100.

Several components of the Texas Heart Institute/Abiomed TAH may be fabricated according to the invention. Thus, high speed components of the centrifugal pump 80 subject to wear may be fabricated from Ti-Nb-Zr alloy and then surface hardened and/or coated with a tightly adherent, hard, wear resistant coating. Further, the rotary valve 100 itself and the surfaces of sleeves 102, 104 and seals 106 may be fabricated from Ti-Nb-Zr alloy then surface hardened or coated with an adherent, wear-resistant coating. Finally, the inner surfaces of the TAH 108, 110 may be fabricated from Ti-Nb-Zr alloys to improve blood compatibility and reduce the potential for thrombus and blood clotting.

The Novacor designed VAD illustrated in FIGS. 9A and B have a solenoid mechanism 120 which sends energy through beam-springs 122, 124 that extend to the back of pump pusher plates 126, 128. The energy stored in the springs translates into linear motion of the plates which exerts force on the flexible blood sac 130. The blood sac 130 consists of a butyl rubber layer sandwiched between two layers of polyurethane Biomer. The blood sac 130 is supported within a cylindrical aluminum ring 132 that acts as a pump housing. The blood inflow 133 and outflow 134 ports are positioned tangentially on opposite sides of the housing to ensure straight-through blood flow. The ports are formed of an epoxy-impregnated Kevlar fabric shell that is integrated into the housing. The ports also encapsulate trileaflet inlet and outlet valves made from bovine pericardium tissue. When implanted into the body, fittings for attaching inflow and outflow valves to vascular conduits are bonded to a pump bulkhead, not shown, which also provides the framework for an encapsulating shell around the pump. This encapsulating shell also has provision for mounting the solenoid energy converter. The solenoid energy converter consists of two solenoid mechanisms, two lightweight titanium beam-springs, and an aluminum support structure. All of these metallic components would come into contact with blood components and body tissue. Therefore, the invention proposes that the titanium beam-springs be replaced with beam-springs of Ti-Nb-Zr alloy. Further, the aluminum support structure would likewise be replaced with a Ti-Nb-Zr alloy support structure that may optionally be hardened and/or coated with a hard coating.

Novacor has identified, in designing the solenoid, that "the challenge was coming up with something that would run for 100 million cycles a year, without requiring maintenance." O'Connor, Lee, "Novacor's VAD: How to Mend a Broken Heart," Mechan. Engr'g pp. 53-55 (Nov. 1991). The invention components fabricated from Ti-Nb-Zr alloys then hardened or coated with hard, wear resistant coatings provide surfaces that are hard, microfretting wear resistant, biocompatible and blood compatible so that they would meet this goal. To further reduce friction and wear of wear surfaces of implant devices, a thin boron of silver surface layer can be applied as an overlay on the previously diffusion hardened Ti-Nb-Zr surface.

External mechanical hearts (EMHs) are used as a bridge to transplant. These hearts include the Jarvik-7 pneumatic heart and the more recent left-ventricular assist device, the Heartmate developed by Thermocardio Systems. In the Heartmate system, two tubes, one carrying air and the other electrical wire, pass from outside the body to an implanted blood pump. The pump is implanted in the abdomen and removes blood from the natural heart's left ventricle. This blood enters and exits the pump through 25 millimeter input and output valves made from chemically processed bovine tissue. The blood flows from the output valve through a dacron-wrapped polyurethane tube to the aorta. An electric motor mounted in the Heartmate's lower chamber actuates a flat-plate piston, which is bonded to a flexible polyurethane diaphragm. When the motor goes through one revolution, it turns a cam assembly that compresses the diaphragm, which pushes blood through the output valve. The operation of the pump is controlled by a microprocessor located in a shoulder bag which adjusts the heartbeat rate by changing the motor's current. According to the invention, the moving parts of the heartmate pump may be replaced with components fabricated from Ti-Nb-Zr alloys then hardened or coated with a hard coating to reduce mechanical wear, friction, and microfretting wear. Furthermore, those metallic components that come into contact with blood components, may also be replaced with Ti-Nb-Zr alloy components similarly coated to improve blood compatibility and reduce the risk of clot formation.

The gravest problem in the use of the pneumatic Jarvik-7 heart has been identified as the formation of blood clots. O'Connor, Lee, "Engineering a Replacement for the Human Heart," Mechan. Engr'g pp. 36-43 (Jul. 1991). In 1990, the FDA withdrew the Jarvik system from clinical trials due to concerns over quality control during manufacture. The University of Utah made modifications to the design of the Jarvik heart to develop a new system called the "Utah 100" which has elliptical pump housings, as opposed to the spherical housings of the Jarvik-7. Further, the Utah 100 has redesigned junctions for joining the diaphragms within the ventricles to the housing. These changes are said to have resulted in an about 70% reduction in blood clot formation relative to the Jarvik-7 design. However, according to the invention, yet further reduction in blood clot formation may be obtained by fabricating moving parts and those metallic surfaces that contact blood components from Ti-Nb-Zr alloys and then hardening and/or coating these components with hard, wear-resistant coating to increase blood compatibility and thrombus resistance, and to reduce abrasive wear, and reduce microfretting wear.

FIGS. 13A and B show, in partial cross section, the distal end of a guide wire fabricated according to the invention. The guide wire 145 has a core 140 of Ti-Nb-Zr alloy with a surface hardened coating 142 to reduce friction which may be further coated with a material that is bio- and hemocompatible and of low friction when in contact with the catheter wall or body tissue. The flexible catheter 146 through which the guide wire moves is also fabricated according to the invention and includes a coil 147 of low modulus titanium alloy which is generally encased by a polymer sheath 148 as shown schematically in FIG. 13C. The guide wire in this case is equipped with a cutting tip 144, preferably also made of Ti-Nb-Zr alloy with a diffusion hardened surface optionally with a hard ceramic or lubricating coating. Since the guide wire is fabricated of metal, it is highly visible under X-rays, providing excellent radiopacity. Boron or silver surface layers may also be deposited on the diffusion hardened surfaces to further reduce friction and wear.

Pacemaker and other electronic leads are manufactured by several corporations, including Medtronic, which produces a range of pacemaker lead designs.

One of these designs is shown in schematic form in FIGS. 14A and B. The pacemaker lead body 150 has a centrally disposed metallic conductor 152 typically made of cobalt-nickel alloy, such as MP35N®. This conductor 152 is usually made up of several strands of wire, each having a diameter of about 0.15-0.20 mm. The conductor 152 is covered by an insulative, protective polymer sheath 153 so that the elongate body 150 of the pacemaker lead has an overall diameter ranging from about 2.2 to about 3 mm. The pacemaker has a first end 154 with an electrode 158 for connecting to a pulse generator and a second end 156 with an electrode 157 for contacting heart muscle. An alternative embodiment is shown in FIG. 14C. As supplied, these two ends are covered with protective polyurethane caps which can be removed for installation of the pacemaker. In order to prevent electrical interference with the conductor 152, a polymeric insulative sleeve 153 is disposed over the entire pacemaker lead body 150, with the exception of the exposed electrodes 157 for contacting heart muscle and the contact electrode 158 for engaging with the pulse generator that houses the electronics and power pack for the pacemaker. As explained before, the organic polymeric sheath compositions, typically polyurethane, can slowly degenerate in the body causing problems, not only due to potential deterioration of electrical insulation and interference with electrical signals but also because of potentially toxic products of degradation.

The invention provides, as shown in FIG. 14C, a pacemaker wherein the conductor 152 is fabricated from a Ti-Nb-Zr alloy that is coated with a tightly adherent, low friction, bio- and hemocompatible coating, with the exception of the electrode for contacting heart muscle 157, and the electrode 158 at the other end of the lead for engaging the pulse generator. The coatings can be formed by in situ oxidation or nitriding of the Ti-Nb-Zr to produce an electrically insulative surface layer of from about 0.1 to about 3 microns in thickness, preferably less than about 0.5 microns in thickness. This process can be carried out at the same time the material is age-hardened. Alternatively, an insulative inert ceramic coating can be applied by conventional CVD or PVD methods either on the original Ti-Nb-Zr alloy surface or onto the diffusion hardened Ti-Nb-Zr surface. For these overlay coatings, the thickness can be as great as 20 microns. The overlay coatings include ceramic metal oxides, metal nitrides, metal carbides, amorphous diamond-like carbon, as detailed above. The electrical signal conductor 152 can comprise either a single wire or multiple wires. Exposed Ti-Nb-Zr metallic ends of the wire or wires are preferably connected directly to a pulse generator thereby avoiding the necessity for a weld or crimp to attach an electrode to the conductor which may result in local galvanic corrosion or physically weakened regions. Further, since the coatings provide a natural protective insulative surface, the use of a coiled construct could be avoided by using only a preferred single-strand, non-coiled low modulus Ti-Nb-Zr metallic wire construct for the conductor 152. This will also eliminate the need for stiff guide wire. Finally, the overall diameter of the pacemaker lead body 150 could be reduced considerably from the range of about 2.2-3 mm for current commercially available leads to about 0.2-1 mm. Optionally, the leads of the invention may be covered with a polymeric sheath.

FIG. 11A shows a schematic of an expandable stent 160, in non-expanded state, positioned on the distal end of a balloon expandable segment 162 of a guide wire 164. The stent is fabricated from Ti-Nb-Zr alloy and is designed so that it can be collapsed over a balloon segment of a balloon catheter. When the stent is in position, within segment of a tubular conduit 165 in the body, a blood vessel for example, to be propped open, the balloon 162 is expanded thereby expanding the stent 160 radially outward up to the blood vessel wall 166 so that means for gripping soft tissue, such as barbs (not shown), on the outer surface of the stent 160 engage and grip blood vessel tissue to anchor the stent 160 in position as shown in FIG. 11B. The balloon 162 is then collapsed and removed leaving the stent in place as shown in FIG. 11C. In this way, the blood vessel is permanently propped open. Urinary, gastrointestinal, and other stent applications are also provided using Ti-Nb-Zr alloy.

FIG. 10 is a representative sketch of a side view of a substantially tubular vascular graft 170 sized to graft onto a blood vessel and made of woven low modulus Ti-Nb-Zr wires 172. While the graft shown is made of woven wires of Ti-Nb-Zr, the graft can also be fabricated from a cylindrical tubing of this alloy. The graft can be fabricated from Ti-Nb-Zr alloy in the lower modulus cold worked condition, or in the slightly higher modulus aged condition with optional surface hardening. Additionally, protein, antibiotic, anti-thrombic, and other surface treatments may be employed to further improve the biocompatibility and clinical performance.

FIGS. 12A and B show a defibrillator including a flexible silicone polymeric patch 300 with a coil of conductive wire 320 (typically titanium, stainless steel, or cobalt-nickel-chromium) on the side of the silicone patch 300 that will contact muscle tissue. When in place in the body, the lead wire 320 that carries power to the coil 340 extends out of the body (through the skin) and is electrically connected to a power source contained in a protective container 360. According to the invention, the lead wire 320 is fabricated with an electrically conductive core 350 of Ti-Nb-Zr alloy and is coated with an adherent electrically insulative coating 380, such as metal oxides, carbides, or nitrides, or with amorphous diamond-like carbon as shown in exaggerated detail FIG. 12B. This coating electrically insulates the lead wire from electrical contact with surrounding body tissue while also protecting the metallic core from corrosion and attack by body fluids, as described previously for the pacemaker lead. Elimination of the polymer coating results in the elimination of potentially toxic products of gradual degradation of the polymer and also the consequent shorting the system when the insulative coating is breached.

The oxygen or nitrogen diffusion hardened surface of the alloy implants may be highly polished to a mirror finish to further improve blood flow characteristics. Further, the oxide- or nitride-coated surfaces maybe coated with substances that enhance biocompatibility and performance. For example, a coating of phosphatidyt choline, heparin, or other proteins to reduce platelet adhesion to the surfaces of the implant, or the use of antibiotic coatings to minimize the potential for infection. Boronated or silver-doped hardened surface layers on the implant reduces friction and wear between contacting parts of heart valves, prosthetic artificial hearts, ventricular assist devices, and other contacting parts in the invention cardiovascular implants. Additionally, amorphous diamond-like carbon, pyrolytic carbon, or other hard ceramic surface layers can also be coated onto the diffusion hardened surface to optimize other friction and wear aspects. The preferred diffusion hardened surface layer described in this application provides a hard, well-attached layer to which these additional hard coatings can be applied with a closer match between substrate and coating with respect to hardness. Other, conventional methods of oxygen surface hardening are also useful. Nitriding of the substrate leads to a hardened nitride surface layer. Methods of nitridation known in the art may be used to achieve a hard nitride layer.

Regardless of how a Ti-Nb-Zr alloy implant's surface is hardened, the friction and wear (tribiological) aspects of the surface can be further improved by employing the use of silver doping or boronation techniques. Ion-beam-assisted deposition of silver films onto ceramic surfaces can improve tribiological behavior. The deposition of up to about 3 microns thick silver films can be performed at room temperature in a vacuum chamber equipped with an electron-beam hard silver evaporation source. A mixture of argon and oxygen gas is fed through the ion source to create an ion flux. One set of acceptable silver deposition parameters consists of an acceleration voltage of 1 key with an ion current density of 25 microamps per cm2. The silver film can be completely deposited by this ion bombardment or formed partially via bombardment while the remaining thickness is achieved by vacuum evaporation. Ion bombardment improves the attachment of the silver film to the Ti-Nb-Zr alloy substrate. Similar deposition of silver films on existing metal cardiovascular implants may also be performed to improve tribological behavior, as well as antibacterial response.

An alternate method to further improve the tribological behavior of Ti-Nb-Zr alloy surfaces of cardiovascular implants is to apply boronation treatments to these surfaces such as commercial available boride vapor deposition, boron ion implantation or sputter deposition using standard ion implantation and evaporation methods, or form a boron-type coating spontaneously in air. Boric Acid (H3 BO3) surface films provide a self-replenishing solid lubricant which can further reduce the friction and wear of the ceramic substrate. These films form from the reaction of the B2 O3 surface (deposited by various conventional methods) on the metal surface with water in the body to form lubricous boric acid. Conventional methods that can be used to deposit either a boron (B), H3 BO3, or B2 O3 surface layer on the cardiovascular implant surface include vacuum evaporation (with or without ion bombardment) or simple oven curing of a thin layer over the implant surface. The self-lubricating mechanism of H3 BO3 is governed by its unique layered, triclinic crystal structure which allows sheets of atoms to easily slide over each other during articulation, thus minimizing substrate wear and friction.

Additionally, surfaces (metal or coated) of all the cardiovascular and medical implants discussed may optionally be coated with agents to further improve biological response. These agents include anticoagulants, proteins, antimicrobial agents, antibiotics, and the like medicaments.

Although the invention has been described with reference to its preferred embodiments, those of ordinary skill in the art may, upon reading this disclosure, appreciate changes and modifications which may be made and which do not depart from the scope and spirit of the invention as described above and claimed below.

Davidson, James A.

Patent Priority Assignee Title
10004584, Jul 10 2006 FIRST QUALITY HYGIENIC, INC Resilient intravaginal device
10034967, Sep 26 2002 VACTRONIX SCIENTIFIC, LLC Implantable biomaterials having engineered functional surfaces
10039866, Sep 26 2002 VACTRONIX SCIENTIFIC, LLC Implantable materials having engineered surfaces and method of making same
10058437, Apr 08 2008 Cook Medical Technologies LLC Surface structure of a component of a medical device and a method of forming the surface structure
10092390, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Method of making implantable medical devices having controlled surface properties
10106884, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Compliant implantable medical devices and methods of making same
10172730, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Stents with metallic covers and methods of making same
10206772, May 09 2011 VACTRONIX SCIENTIFIC, LLC Implantable medical device having enhanced endothelial migration features and methods of making the same
10219884, Jul 10 2006 FIRST QUALITY HYGIENIC, INC Resilient device
10292849, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Balloon catheter having metal balloon and method of making same
10314949, Sep 26 2002 VACTRONIX SCIENTIFIC, LLC Implantable biomaterials having functional surfaces
10357354, May 12 2000 VACTRONIX SCIENTIFIC, LLC Monolithic biocompatible implantable laminated materials
10363125, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Method of making implantable medical devices having controlled surface properties
10449030, May 12 2000 VACTRONIX SCIENTIFIC, LLC Self-supporting laminated films, structural materials and medical devices manufactured therefrom and methods of making same
10465274, Sep 26 2002 VACTRONIX SCIENTIFIC, LLC Implantable graft and methods of making same
10682171, Jun 28 2006 Medtronic Cryocath LP Variable geometry cooling chamber
10682443, Sep 26 2002 VACTRONIX SCIENTIFIC, LLC Implantable biomaterials having functional surfaces
10729824, Sep 26 2002 VACTRONIX SCIENTIFIC, LLC Implantable materials having engineered surfaces and method of making same
10745799, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Compliant implantable medical devices and methods of making same
10786343, May 09 2011 VACTRONIX SCIENTIFIC, LLC Implantable medical device having enhanced endothelial migration features and methods of making the same
10849652, Oct 05 2010 Emory University Devices, systems, and methods for improving access to cardiac and vascular chambers
10874532, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Implantable medical devices having controlled surface properties for improved healing response
10939991, May 12 2000 VACTRONIX SCIENTIFIC, LLC Monolithic biocompatible implantable laminated materials
10945828, May 12 2000 VACTRONIX SCIENTIFIC, LLC Self-supporting laminated films, structural materials and medical devices manufactured therefrom and methods of making same
11633225, Jun 28 2006 Medtronic Cryocath LP Variable geometry cooling chamber
5891192, May 22 1997 Regents of the University of California, The Ion-implanted protein-coated intralumenal implants
5902317, Jun 01 1994 NMT MEDICAL, INC Stent and method and apparatus for forming and delivering the same
6159219, May 16 1997 Boston Scientific Scimed, Inc Stent retrieval device
6187037, Mar 11 1998 Metal stent containing radioactivatable isotope and method of making same
6287332, Jun 25 1998 BIOTRONIK AG Implantable, bioresorbable vessel wall support, in particular coronary stent
6290721, Mar 31 1992 Boston Scientific Scimed, Inc Tubular medical endoprostheses
6379383, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Endoluminal device exhibiting improved endothelialization and method of manufacture thereof
6402787, Jan 30 2000 DIMICRON, INC Prosthetic hip joint having at least one sintered polycrystalline diamond compact articulation surface and substrate surface topographical features in said polycrystalline diamond compact
6402859, Sep 10 1999 TERUMO CORPORATION A JAPANESE CORPORATION; TOKUSEN KOGYO CO , LTD A JAPANESE CORPORATION β-titanium alloy wire, method for its production and medical instruments made by said β-titanium alloy wire
6494918, Jan 30 2000 DIMICRON, INC Component for a prosthetic joint having a diamond load bearing and articulation surface
6514289, Jan 30 2000 DIMICRON, INC Diamond articulation surface for use in a prosthetic joint
6517583, Jan 30 2000 DIMICRON, INC Prosthetic hip joint having a polycrystalline diamond compact articulation surface and a counter bearing surface
6520923, Jun 17 1998 Advanced Cardiovascular Systems, Inc. Performance enhancing coating on intraluminal devices
6537310, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Endoluminal implantable devices and method of making same
6572651, Jun 03 1998 BLUE MEDICAL DEVICES B V Stents with a diamond like coating
6582652, May 11 2001 Boston Scientific Scimed, Inc Stainless steel alloy having lowered nickel-chromium toxicity and improved biocompatibility
6596225, Jan 31 2000 DIMICRON, INC Methods for manufacturing a diamond prosthetic joint component
6610095, Jan 30 2000 DIMICRON, INC Prosthetic joint having substrate surface topographical featurers and at least one diamond articulation surface
6635082, Dec 29 2000 Advanced Cardiovascular Systems, INC Radiopaque stent
6641607, Dec 29 2000 Advanced Cardiovascular Systems, INC Double tube stent
6676704, Jan 30 2000 DIMICRON, INC Prosthetic joint component having at least one sintered polycrystalline diamond compact articulation surface and substrate surface topographical features in said polycrystalline diamond compact
6695865, Mar 20 2000 VACTRONIX SCIENTIFIC, LLC Embolic protection device
6709463, Jan 30 2000 DIMICRON, INC Prosthetic joint component having at least one solid polycrystalline diamond component
6733513, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Balloon catheter having metal balloon and method of making same
6793681, Aug 12 1994 DIMICRON, INC Prosthetic hip joint having a polycrystalline diamond articulation surface and a plurality of substrate layers
6800095, Aug 12 1994 DIMICRON, INC Diamond-surfaced femoral head for use in a prosthetic joint
6800153, Sep 10 1999 Terumo Corporation; TOKUSEN KOGYO CO., LTD. Method for producing β-titanium alloy wire
6820676, Nov 04 1999 VACTRONIX SCIENTIFIC, LLC Endoluminal device exhibiting improved endothelialization and method of manufacture thereof
6849085, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Self-supporting laminated films, structural materials and medical devices manufactured therefrom and method of making same
6869701, Aug 16 1999 AITA, CAROLYN Self-repairing ceramic coatings
6913762, Apr 25 2001 Mayo Foundation for Medical Education and Research Stent having non-woven framework containing cells
6936066, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Complaint implantable medical devices and methods of making same
6938668, Jan 25 2000 Boston Scientific Scimed, Inc Manufacturing medical devices by vapor deposition
7077867, Aug 12 1994 DIMICRON, INC Prosthetic knee joint having at least one diamond articulation surface
7101392, Mar 21 1992 Boston Scientific Scimed, Inc Tubular medical endoprostheses
7160317, Jan 04 2002 Boston Scientific Scimed, Inc Multiple-wing balloon catheter to reduce damage to coated expandable medical implants
7163715, Jun 12 2001 Advanced Cardiovascular Systems, INC Spray processing of porous medical devices
7195641, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Valvular prostheses having metal or pseudometallic construction and methods of manufacture
7201940, Jun 12 2001 Advanced Cardiovascular Systems, Inc. Method and apparatus for thermal spray processing of medical devices
7235092, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Guidewires and thin film catheter-sheaths and method of making same
7300457, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Self-supporting metallic implantable grafts, compliant implantable medical devices and methods of making same
7396501, Jun 01 1995 DIMICRON, INC Use of gradient layers and stress modifiers to fabricate composite constructs
7396505, Aug 12 1994 DIMICRON, INC Use of CoCrMo to augment biocompatibility in polycrystalline diamond compacts
7396538, Sep 26 2002 Endovascular Devices, Inc.; ENDOVASCULAR DEVICES, INC Apparatus and method for delivery of mitomycin through an eluting biocompatible implantable medical device
7442207, Apr 21 2006 Medtronic Vascular, Inc. Device, system, and method for treating cardiac valve regurgitation
7445749, May 11 2001 Boston Scientific Scimed, Inc Stainless steel alloy having lowered nickel chromium toxicity and improved biocompatibility
7491226, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Endoluminal implantable stent-grafts
7494507, Jan 30 2000 DIMICRON, INC Articulating diamond-surfaced spinal implants
7514122, Jun 12 2001 Advanced Cardiovascular Systems, Inc. Method and apparatus for spray processing of porous medical devices
7625594, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Endoluminal device exhibiting improved endothelialization and method of manufacture thereof
7641680, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Endoluminal implantable stent-grafts
7641682, Jul 03 2001 VACTRONIX SCIENTIFIC, LLC Compliant implantable medical devices and methods of making same
7704274, Sep 26 2002 VACTRONIX SCIENTIFIC, LLC Implantable graft and methods of making same
7713297, Aug 29 2003 Boston Scientific Scimed, Inc Drug-releasing stent with ceramic-containing layer
7717892, Jul 10 2006 FIRST QUALITY HYGIENIC, INC Method of treating urinary incontinence
7727273, Jan 13 2005 Boston Scientific Scimed, Inc. Medical devices and methods of making the same
7736687, Jan 31 2006 VACTRONIX SCIENTIFIC, LLC Methods of making medical devices
7833284, Jun 28 2006 CLEVELAND CLINIC FOUNDATION, THE Anti-adhesion membrane
7854756, Jan 22 2004 Boston Scientific Scimed, Inc Medical devices
7854958, Jun 12 2001 Advanced Cardiovascular Systems, Inc. Method and apparatus for spray processing of porous medical devices
7892163, Jul 10 2006 FIRST QUALITY HYGIENIC, INC Method of treating urinary incontinence
7931683, Jul 27 2007 Boston Scientific Scimed, Inc. Articles having ceramic coated surfaces
7938854, Jan 13 2005 Boston Scientific Scimed, Inc. Medical devices and methods of making the same
7938855, Nov 02 2007 Boston Scientific Scimed, Inc Deformable underlayer for stent
7942926, Jul 11 2007 Boston Scientific Scimed, Inc Endoprosthesis coating
7955382, Sep 15 2006 Boston Scientific Scimed, Inc. Endoprosthesis with adjustable surface features
7976915, May 23 2007 Boston Scientific Scimed, Inc Endoprosthesis with select ceramic morphology
7981150, Nov 09 2006 Boston Scientific Scimed, Inc Endoprosthesis with coatings
7985252, Jul 30 2008 Boston Scientific Scimed, Inc. Bioerodible endoprosthesis
7998192, May 09 2008 Boston Scientific Scimed, Inc. Endoprostheses
8002821, Sep 18 2006 Boston Scientific Scimed, Inc. Bioerodible metallic ENDOPROSTHESES
8002823, Jul 11 2007 Boston Scientific Scimed, Inc Endoprosthesis coating
8029554, Nov 02 2007 Boston Scientific Scimed, Inc Stent with embedded material
8043366, Sep 08 2005 Boston Scientific Scimed, Inc. Overlapping stent
8047980, Jul 10 2006 FIRST QUALITY HYGIENIC, INC Method of treating urinary incontinence
8048143, Jan 22 2004 Boston Scientific Scimed, Inc. Medical devices
8048150, Apr 12 2006 Boston Scientific Scimed, Inc. Endoprosthesis having a fiber meshwork disposed thereon
8052743, Aug 02 2006 Boston Scientific Scimed, Inc Endoprosthesis with three-dimensional disintegration control
8052744, Sep 15 2006 Boston Scientific Scimed, Inc. Medical devices and methods of making the same
8052745, Sep 13 2007 Boston Scientific Scimed, Inc Endoprosthesis
8057534, Sep 15 2006 Boston Scientific Scimed, Inc Bioerodible endoprostheses and methods of making the same
8066763, Apr 11 1998 Boston Scientific Scimed, Inc. Drug-releasing stent with ceramic-containing layer
8067054, Apr 05 2007 Boston Scientific Scimed, Inc. Stents with ceramic drug reservoir layer and methods of making and using the same
8070797, Mar 01 2007 Boston Scientific Scimed, Inc Medical device with a porous surface for delivery of a therapeutic agent
8071155, May 05 2005 Boston Scientific Scimed, Inc. Medical devices and methods of making the same
8071156, Mar 04 2009 Boston Scientific Scimed, Inc. Endoprostheses
8080055, Dec 28 2006 Boston Scientific Scimed, Inc Bioerodible endoprostheses and methods of making the same
8089029, Feb 01 2006 Boston Scientific Scimed, Inc. Bioabsorbable metal medical device and method of manufacture
8128689, Sep 15 2006 Boston Scientific Scimed, Inc Bioerodible endoprosthesis with biostable inorganic layers
8137614, Sep 26 2003 Boston Scientific Scimed, Inc. Medical devices and method for making the same
8147859, Mar 28 2005 VACTRONIX SCIENTIFIC, LLC Implantable material having patterned surface of raised elements and photochemically altered elements and method of making same
8177706, Jul 10 2006 FIRST QUALITY HYGIENIC, INC Method of treating urinary incontinence
8187320, Feb 16 2001 YAMANOUCHI PHARMACEUTICAL CO , LTD ; Astellas Pharma INC Medical implants containing FK506 (tacrolimus)
8187620, Mar 27 2006 Boston Scientific Scimed, Inc. Medical devices comprising a porous metal oxide or metal material and a polymer coating for delivering therapeutic agents
8216632, Nov 02 2007 Boston Scientific Scimed, Inc Endoprosthesis coating
8221822, Jul 31 2007 Boston Scientific Scimed, Inc Medical device coating by laser cladding
8231980, Dec 03 2008 Boston Scientific Scimed, Inc Medical implants including iridium oxide
8236014, Jun 14 2004 Edwards Lifesciences Corporation Methods for arterio-venous fistula creation
8236046, Jun 10 2008 Boston Scientific Scimed, Inc. Bioerodible endoprosthesis
8247020, Jan 31 2006 VACTRONIX SCIENTIFIC, LLC Methods of making medical devices
8267992, Mar 02 2009 Boston Scientific Scimed, Inc Self-buffering medical implants
8268340, Sep 26 2002 VACTRONIX SCIENTIFIC, LLC Implantable materials having engineered surfaces and method of making same
8287937, Apr 24 2009 Boston Scientific Scimed, Inc. Endoprosthese
8303643, Nov 19 2003 Remon Medical Technologies Ltd. Method and device for electrochemical formation of therapeutic species in vivo
8313523, May 07 2003 VACTRONIX SCIENTIFIC, LLC Metallic implantable grafts and method of making same
8329202, Nov 12 2004 DEPUY SYNTHES PRODUCTS, INC System and method for attaching soft tissue to an implant
8349249, Feb 10 2003 HERAEUS DEUTSCHLAND GMBH & CO KG Metal alloy for medical devices and implants
8353949, Sep 14 2006 Boston Scientific Scimed, Inc. Medical devices with drug-eluting coating
8382824, Oct 03 2008 Boston Scientific Scimed, Inc. Medical implant having NANO-crystal grains with barrier layers of metal nitrides or fluorides
8399008, Nov 12 2004 Purdue Research Foundation System and method for attaching soft tissue to annodized metal implant
8403980, Feb 10 2003 HERAEUS DEUTSCHLAND GMBH & CO KG Metal alloy for medical devices and implants
8431149, Mar 01 2007 Boston Scientific Scimed, Inc Coated medical devices for abluminal drug delivery
8449603, Jun 18 2008 Boston Scientific Scimed, Inc Endoprosthesis coating
8458879, Jul 03 2001 VACTRONIX SCIENTIFIC, LLC Method of fabricating an implantable medical device
8460333, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Balloon catheter having metal balloon and method of making same
8460361, Jan 25 2000 Boston Scientific Scimed, Inc. Manufacturing medical devices by vapor deposition
8574615, Mar 24 2006 Boston Scientific Scimed, Inc. Medical devices having nanoporous coatings for controlled therapeutic agent delivery
8580189, May 11 2001 Boston Scientific Scimed, Inc. Stainless steel alloy having lowered nickel-chrominum toxicity and improved biocompatibility
8608639, Jul 10 2006 FIRST QUALITY HYGIENIC, INC Resilient device
8613698, Jul 10 2006 FIRST QUALITY HYGIENIC, INC Resilient device
8617238, Aug 17 2010 VACTRONIX SCIENTIFIC, LLC Transluminal cardiac ball valve and method for deployment thereof
8632583, May 09 2011 VACTRONIX SCIENTIFIC, LLC Implantable medical device having enhanced endothelial migration features and methods of making the same
8641747, Jun 14 2004 Edwards Lifesciences Corporation Devices for arterio-venous fistula creation
8641754, Nov 07 2000 VACTRONIX SCIENTIFIC, LLC Endoluminal stent, self-supporting endoluminal graft and methods of making same
8647700, Jan 31 2006 VACTRONIX SCIENTIFIC, LLC Methods of making medical devices
8668732, Mar 23 2010 Boston Scientific Scimed, Inc. Surface treated bioerodible metal endoprostheses
8679517, Sep 26 2002 VACTRONIX SCIENTIFIC, LLC Implantable materials having engineered surfaces made by vacuum deposition and method of making same
8709066, Sep 26 2002 VACTRONIX SCIENTIFIC, LLC Implantable materials having engineered surfaces comprising a pattern of features and method of making same
8715335, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Endoluminal implantable stent-grafts
8715339, Dec 28 2006 Boston Scientific Scimed, Inc. Bioerodible endoprostheses and methods of making the same
8728563, May 03 2011 VACTRONIX SCIENTIFIC, LLC Endoluminal implantable surfaces, stents, and grafts and method of making same
8753258, Jul 10 2006 FIRST QUALITY HYGIENIC, INC Resilient device
8771343, Jun 29 2006 Boston Scientific Scimed, Inc. Medical devices with selective titanium oxide coatings
8808726, Sep 15 2006 Boston Scientific Scimed, Inc Bioerodible endoprostheses and methods of making the same
8815273, Jul 27 2007 Boston Scientific Scimed, Inc. Drug eluting medical devices having porous layers
8815275, Jun 28 2006 Boston Scientific Scimed, Inc. Coatings for medical devices comprising a therapeutic agent and a metallic material
8840660, Jan 05 2006 Boston Scientific Scimed, Inc.; Boston Scientific Scimed, Inc Bioerodible endoprostheses and methods of making the same
8845713, May 12 2000 VACTRONIX SCIENTIFIC, LLC Self-supporting laminated films, structural materials and medical devices manufactured therefrom and methods of making same
8900292, Aug 03 2007 Boston Scientific Scimed, Inc Coating for medical device having increased surface area
8910363, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Compliant implantable medical devices and methods of making same
8920491, Apr 22 2008 Boston Scientific Scimed, Inc. Medical devices having a coating of inorganic material
8932346, Apr 24 2008 Boston Scientific Scimed, Inc. Medical devices having inorganic particle layers
8932347, Sep 26 2002 VACTRONIX SCIENTIFIC, LLC Implantable materials having engineered surfaces and method of making same
8945601, Nov 12 2004 DEPUY SYNTHES PRODUCTS, INC System and method for attaching soft tissue to an implant
9050183, Jul 10 2006 FIRST QUALITY HYGIENIC, INC Resilient device
9132001, May 07 2003 VACTRONIX SCIENTIFIC, LLC Metallic implantable grafts and method of making same
9173768, Jul 10 2006 FIRST QUALITY HYGIENIC, INC Resilient device
9173983, Apr 08 2008 Cook Medical Technologies LLC Surface structure of a component of a medical device and a method of forming the surface structure
9272077, Sep 26 2002 VACTRONIX SCIENTIFIC, LLC Implantable materials having engineered surfaces and method of making same
9284409, Jul 19 2007 Boston Scientific Scimed, Inc Endoprosthesis having a non-fouling surface
9284637, Sep 26 2002 VACTRONIX SCIENTIFIC, LLC Implantable graft and methods of making same
9320626, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Guidewires and thin film catheter-sheaths and method of making same
9375330, Jan 31 2006 VACTRONIX SCIENTIFIC, LLC Methods of making medical devices
9439789, May 09 2011 VACTRONIX SCIENTIFIC, LLC Implantable medical device having enhanced endothelial migration features and methods of making the same
9463305, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Balloon catheter having metal balloon and method of making same
9498218, Nov 12 2004 Purdue Research Foundation; DePuy Synthes Products, Inc. System and method for attaching soft tissue to an implant comprising a nanotextured surface
9566148, May 12 2000 VACTRONIX SCIENTIFIC, LLC Self-supporting laminated films, structural materials and medical devices manufactured therefrom and methods of making same
9662230, Nov 19 1999 VACTRONIX SCIENTIFIC, LLC Implantable medical devices having controlled surface properties for improved healing response
9814511, Jun 28 2006 Medtronic Cryocath LP Variable geometry cooling chamber
Patent Priority Assignee Title
2892706,
2987352,
3370946,
3408604,
3643658,
3677795,
3752664,
3777346,
3849124,
3906550,
3911783,
4040129, Jul 15 1970 Institut Dr. Ing. Reinhard Straumann AG Surgical implant and alloy for use in making an implant
4145764, Jul 23 1975 Sumitomo Chemical Co., Ltd.; Matsumoto Dental College Endosseous implants
4170990, Jan 28 1977 FRIED. KRUPP Gesellschaft mit beschrankter Haftung Method for implanting and subsequently removing mechanical connecting elements from living tissue
4197643, Mar 14 1978 University of Connecticut Orthodontic appliance of titanium alloy
4511411, Sep 07 1982 Vereinigte Drahtwerke AG Method of forming a hard surface layer on a metal component
4778461, Nov 23 1985 Beiersdorf AG Heart valve prosthesis and process for its production
4857269, Sep 09 1988 HOWMEDICA OSTEONICS CORP High strength, low modulus, ductile, biopcompatible titanium alloy
4902359, May 18 1986 Daido Tokushuko Kabushiki Kaisha; Fuji Valve Co., Ltd. Wear-resistant titanium or titanium-alloy member and a method for manufacturing the same
4983184, Oct 16 1987 Institut Straumann AG Alloplastic material for producing an artificial soft tissue component and/or for reinforcing a natural soft tissue component
5169597, Dec 21 1989 HOWMEDICA OSTEONICS CORP Biocompatible low modulus titanium alloy for medical implants
5195984, Oct 04 1988 CARDINAL HEALTH SWITZERLAND 515 GMBH Expandable intraluminal graft
5197978, Apr 26 1991 United States Surgical Corporation Removable heat-recoverable tissue supporting device
DE2703529,
EP437079A1,
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